Your search keyword '"Palasiewicz K"' showing total 22 results

1. MAFB enhances oncogenic Notch signaling in T cell acute lymphoblastic leukemia

Author

Pajcini, K.V. (Kostandin V.), Xu, L. (Liang), Shao, L. (Lijian), Petrovic, J. (Jelena), Palasiewicz, K. (Karol), Ohtani, Y. (Yumi), Bailis, W. (Will), Lee, C. (Curtis), Wertheim, G. (Gerald), Mani, R. (Rajeswaran), Musuthamy, N. (Natarajan), Li, Y. (Yunlei), Meijerink, J.P.P. (Jules), Blacklow, S.C. (Stephen C.), Faryabi, R.B. (Robert B.), Cherry, S. (Sara), Pear, W.S. (Warren), Pajcini, K.V. (Kostandin V.), Xu, L. (Liang), Shao, L. (Lijian), Petrovic, J. (Jelena), Palasiewicz, K. (Karol), Ohtani, Y. (Yumi), Bailis, W. (Will), Lee, C. (Curtis), Wertheim, G. (Gerald), Mani, R. (Rajeswaran), Musuthamy, N. (Natarajan), Li, Y. (Yunlei), Meijerink, J.P.P. (Jules), Blacklow, S.C. (Stephen C.), Faryabi, R.B. (Robert B.), Cherry, S. (Sara), and Pear, W.S. (Warren)

Abstract

Activating mutations in the gene encoding the cell-cell contact signaling protein Notch1 are common in human T cell acute lymphoblastic leukemias (T-ALLs). However, expressing Notch1 mutant alleles in mice fails to efficiently induce the develop

Published

2017

2. Dysregulation of IL-34 ligation to SDC-1 mitigates collagen-induced arthritis.

Author

Meyer A, Sienes R, Zanotti B, van Raemdonck K, Palasiewicz K, Mass DP, Volin MV, and Shahrara S

Subjects

Animals, Humans, Tumor Necrosis Factor-alpha, Arthritis, Experimental, Arthritis, Rheumatoid

Published

2022

3. Phosphatidylserine externalization by apoptotic cells is dispensable for specific recognition leading to innate apoptotic immune responses.

Author

Gomes MT, Palasiewicz K, Gadiyar V, Lahey K, Calianese D, Birge RB, and Ucker DS

Subjects

Animals, Cell Line, Humans, Immunomodulation, Mice, Apoptosis physiology, Immunity, Innate, Phagocytosis physiology, Phosphatidylserines metabolism

Abstract

Surface determinants newly expressed by apoptotic cells that are involved in triggering potent immunosuppressive responses, referred to as "innate apoptotic immunity (IAI)" have not been characterized fully. It is widely assumed, often implicitly, that phosphatidylserine, a phospholipid normally cloistered in the inner leaflet of cells and externalized specifically during apoptosis, is involved in triggering IAI, just as it plays an essential role in the phagocytic recognition of apoptotic cells. It is notable, however, that the triggering of IAI in responder cells is not dependent on the engulfment of apoptotic cells by those responders. Contact between the responder and the apoptotic target, on the other hand, is necessary to elicit IAI. Previously, we demonstrated that exposure of protease-sensitive determinants on the apoptotic cell surface are essential for initiating IAI responses; exposed glycolytic enzyme molecules were implicated in particular. Here, we report our analysis of the involvement of externalized phosphatidylserine in triggering IAI. To analyze the role of phosphatidylserine, we employed a panel of target cells that either externalized phosphatidylserine constitutively, independently of apoptosis, or did not, as well as their WT parental cells that externalized the phospholipid in an apoptosis-dependent manner. We found that the externalization of phosphatidylserine, which can be fully uncoupled from apoptosis, is neither sufficient nor necessary to trigger the profound immunomodulatory effects of IAI. These results reinforce the view that apoptotic immunomodulation and phagocytosis are dissociable and further underscore the significance of protein determinants localized to the cell surface during apoptosis in triggering innate apoptotic immunity., Competing Interests: Conflict of interest The authors declare that they have no conflicts of interest with the contents of this article., (Copyright © 2022 The Authors. Published by Elsevier Inc. All rights reserved.)

Published

2022

4. Inhibition of IRAK4 dysregulates SARS-CoV-2 spike protein-induced macrophage inflammatory and glycolytic reprogramming.

Author

Umar S, Palasiewicz K, Meyer A, Kumar P, Prabhakar BS, Volin MV, Rahat R, Al-Awqati M, Chang HJ, Zomorrodi RK, Rehman J, and Shahrara S

Subjects

Angiotensin-Converting Enzyme 2, Animals, HEK293 Cells, Humans, Interferon Regulatory Factors metabolism, Interferon Regulatory Factors pharmacology, Interleukin-1 Receptor-Associated Kinases genetics, Interleukin-1 Receptor-Associated Kinases metabolism, Macrophages metabolism, Mice, SARS-CoV-2, Toll-Like Receptor 2 metabolism, Toll-Like Receptor 7 metabolism, COVID-19, Spike Glycoprotein, Coronavirus genetics, Spike Glycoprotein, Coronavirus metabolism

Abstract

Escalated innate immunity plays a critical role in SARS-CoV-2 pathology; however, the molecular mechanism is incompletely understood. Thus, we aim to characterize the molecular mechanism by which SARS-CoV-2 Spike protein advances human macrophage (Mϴ) inflammatory and glycolytic phenotypes and uncover novel therapeutic strategies. We found that human Mϴs exposed to Spike protein activate IRAK4 phosphorylation. Blockade of IRAK4 in Spike protein-stimulated Mϴs nullifies signaling of IRAK4, AKT, and baseline p38 without affecting ERK and NF-κB activation. Intriguingly, IRAK4 inhibitor (IRAK4i) rescues the SARS-CoV-2-induced cytotoxic effect in ACE2 + HEK 293 cells. Moreover, the inflammatory reprogramming of Mϴs by Spike protein was blunted by IRAK4i through IRF5 and IRF7, along with the reduction of monokines, IL-6, IL-8, TNFα, and CCL2. Notably, in Spike protein-stimulated Mϴs, suppression of the inflammatory markers by IRAK4i was coupled with the rebalancing of oxidative phosphorylation over metabolic activity. This metabolic adaptation promoted by IRAK4i in Spike protein-activated Mϴs was shown to be in part through constraining PFKBF3, HIF1α, cMYC, LDHA, lactate expression, and reversal of citrate and succinate buildup. IRAK4 knockdown could comparably impair Spike protein-enhanced inflammatory and metabolic imprints in human Mϴs as those treated with ACE2, TLR2, and TLR7 siRNA. Extending these results, in murine models, where human SARS-CoV-2 Spike protein was not recognized by mouse ACE2, TLRs were responsible for the inflammatory and glycolytic responses instigated by Spike protein and were dysregulated by IRAK4i therapy. In conclusion, IRAK4i may be a promising strategy for severe COVID-19 patients by counter-regulating ACE2 and TLR-mediated Mϴ hyperactivation. IRAK4i therapy counteracts Mϴ inflammatory and glycolytic reprogramming triggered by Spike protein. This study illustrates that SARS-CoV-2 Spike protein activates IRAK4 signaling via ACE2 as well as TLR2 and TLR7 sensing in human Mϴs. Remarkably, IRAK4i treatment can dysregulate both ACE-dependent and independent (via TLR sensing) SARS-CoV-2 Spike protein-activated inflammatory and metabolic imprints., (© 2022. The Author(s), under exclusive licence to Springer Nature Switzerland AG.)

Published

2022

5. Metabolic reprogramming of macrophages instigates CCL21-induced arthritis.

Author

Van Raemdonck K, Umar S, Palasiewicz K, Meyer A, Volin MV, Chang HJ, Al-Awqati M, Zomorrodi RK, and Shahrara S

Subjects

Animals, Glycolysis, Interleukin-6 metabolism, Mice, Tumor Necrosis Factor-alpha metabolism, Arthritis, Rheumatoid metabolism, Macrophages metabolism

Abstract

This study was designed to delineate the functional significance of CCL21 in metabolic reprogramming in experimental arthritis and differentiated rheumatoid arthritis (RA) macrophages (MΦs). To characterize the influence of CCL21 on immunometabolism, its mechanism of action was elucidated by dysregulating glucose uptake in preclinical arthritis and RA MΦs. In CCL21 arthritic joints, the glycolytic intermediates hypoxia-inducible factor 1α (HIF1α), cMYC and GLUT1 were overexpressed compared with oxidative regulators estrogen-related receptor γ and peroxisome proliferator-activated receptor gamma coactivator 1 (PGC1)-α. Interestingly, 2-deoxy-D-glucose (2-DG) therapy mitigated CCL21-induced arthritis by restraining the number of joint F4/80 + iNOS + MΦs without impacting F4/80 + Arginase + MΦs. Similar to the preclinical findings, blockade of glycolysis negated CCL21-polarized CD14 + CD86 + GLUT + MΦ frequency; however, CD14 + CD206 + GLUT + MΦs were not implicated in this process. In CCL21-induced arthritis and differentiated RA MΦs, the inflammatory imprint was uniquely intercepted by 2-DG via interleukin-6 (IL-6) downregulation. Despite the more expansive inflammatory response of CCL21 in the arthritic joints relative to the differentiated RA MΦs, 2-DG was ineffective in joint tumor necrosis factor-α, IL-1β, CCL2 and CCL5 enrichment. By contrast, disruption of glycolysis markedly impaired CCL21-induced HIF1α and cMYC signaling in arthritic mice. Notably, in RA MΦs, glycolysis interception was directed toward dysregulating CCL21-enhanced HIF1α transcription. Nonetheless, in concurrence with the diminished IL-6 levels, CCL21 differentiation of CD14 + CD86 + GLUT1 + MΦs was reversed by glycolysis and HIIF1α inhibition. Moreover, in the CCL21 experimental arthritis or differentiated RA MΦs, the malfunctioning metabolic machinery was accompanied by impaired oxidative phosphorylation because of reduced PGC1α or peroxisome proliferator-activated receptor-γ expression. CCL21 reconfigures naïve myeloid cells into glycolytic RA CD14 + CD86 + GLUT + IL-6 high HIF1α high MΦs. Therefore, inhibiting the CCL21/CCR7 pathway may provide a promising therapeutic strategy., (© 2021 Australian and New Zealand Society for Immunology, Inc.)

Published

2022

6. IRAK4 inhibitor mitigates joint inflammation by rebalancing metabolism malfunction in RA macrophages and fibroblasts.

Author

Umar S, Palasiewicz K, Volin MV, Zanotti B, Al-Awqati M, Sweiss N, and Shahrara S

Subjects

Adjuvants, Immunologic pharmacology, Adjuvants, Immunologic therapeutic use, Animals, Arthritis, Rheumatoid drug therapy, Cells, Cultured, Fibroblasts drug effects, Humans, Imiquimod pharmacology, Imiquimod therapeutic use, Inflammation drug therapy, Inflammation metabolism, Inflammation Mediators antagonists & inhibitors, Interleukin-1 Receptor-Associated Kinases antagonists & inhibitors, Macrophages drug effects, Mice, Mice, Inbred DBA, Arthritis, Rheumatoid metabolism, Fibroblasts metabolism, Inflammation Mediators metabolism, Interleukin-1 Receptor-Associated Kinases metabolism, Macrophages metabolism

Abstract

Recent studies show a connection between glycolysis and inflammatory response in rheumatoid arthritis (RA) macrophages (MΦs) and fibroblasts (FLS). Yet, it is unclear which pathways could be targeted to rebalance RA MΦs and FLS metabolic reprogramming. To identify novel targets that could normalize RA metabolic reprogramming, TLR7-mediated immunometabolism was characterized in RA MΦs, FLS and experimental arthritis. We uncovered that GLUT1, HIF1α, cMYC, LDHA and lactate were responsible for the TLR7-potentiated metabolic rewiring in RA MΦs and FLS, which was negated by IRAK4i. While in RA FLS, HK2 was uniquely expanded by TLR7 and negated by IRAK4i. Conversely, TLR7-driven hypermetabolism, non-oxidative PPP (CARKL) and oxidative phosphorylation (PPARγ) were narrowly dysregulated in TLR7-activated RA MΦs and FLS and was reversed by IRAK4i. Consistently, IRAK4i therapy disrupted arthritis mediated by miR-Let7b/TLR7 along with impairing a broad-range of glycolytic intermediates, GLUT1, HIF1α, cMYC, HK2, PFKFB3, PKM2, PDK1 and RAPTOR. Notably, inhibition of the mutually upregulated glycolytic metabolites, HIF1α and cMYC, was capable of mitigating TLR7-induced inflammatory imprint in RA MΦs and FLS. In keeping with IRAK4i, treatment with HIF1i and cMYCi intercepted TLR7-enhanced IRF5 and IRF7 in RA MΦs, distinct from RA FLS. Interestingly, in RA MΦs and FLS, IRAK4i counteracted TLR7-induced CARKL reduction in line with HIF1i. Whereas, cMYCi in concordance with IRAK4i, overturned oxidative phosphorylation via PPARγ in TLR7-activated RA MΦs and FLS. The blockade of IRAK4 and its interconnected intermediates can rebalance the metabolic malfunction by obstructing glycolytic and inflammatory phenotypes in RA MΦs and FLS., (Copyright © 2021 Elsevier Inc. All rights reserved.)

Published

2021

7. Metabolic regulation of RA macrophages is distinct from RA fibroblasts and blockade of glycolysis alleviates inflammatory phenotype in both cell types.

Author

Umar S, Palasiewicz K, Volin MV, Romay B, Rahat R, Tetali C, Arami S, Guma M, Ascoli C, Sweiss N, Zomorrodi RK, O'Neill LAJ, and Shahrara S

Subjects

Animals, Antimetabolites pharmacology, Arthritis, Experimental physiopathology, Cell Movement, Cytokines, Fibroblasts drug effects, Fibroblasts metabolism, Fibroblasts pathology, Humans, Inflammation etiology, Inflammation metabolism, Inflammation pathology, Macrophages drug effects, Macrophages metabolism, Macrophages pathology, Mice, Mice, Inbred DBA, Pentose Phosphate Pathway, Phenotype, Arthritis, Rheumatoid physiopathology, Deoxyglucose pharmacology, Fibroblasts immunology, Glycolysis, Inflammation prevention & control, Macrophages immunology, Th17 Cells immunology

Abstract

Recent studies have shown the significance of metabolic reprogramming in immune and stromal cell function. Yet, the metabolic reconfiguration of RA macrophages (MΦs) is incompletely understood during active disease and in crosstalk with other cell types in experimental arthritis. This study elucidates a distinct regulation of glycolysis and oxidative phosphorylation in RA MΦs compared to fibroblast (FLS), although PPP (Pentose Phosphate pathway) is similarly reconfigured in both cell types. 2-DG treatment showed a more robust impact on impairing the RA M1 MΦ-mediated inflammatory phenotype than IACS-010759 (IACS, complexli), by reversing ERK, AKT and STAT1 signaling, IRF8/3 transcription and CCL2 or CCL5 secretion. This broader inhibitory effect of 2-DG therapy on RA M1 MΦs was linked to dysregulation of glycolysis (GLUT1, PFKFB3, LDHA, lactate) and oxidative PPP (NADP conversion to NADPH), while both compounds were ineffective on oxidative phosphorylation. Distinctly, in RA FLS, 2-DG and IACS therapies constrained LPS/IFNγ-induced AKT and JNK signaling, IRF5/7 and fibrokine expression. Disruption of RA FLS metabolic rewiring by 2-DG or IACS therapy was accompanied by a reduction of glycolysis (HIF1α, PFKFB3) and suppression of citrate or succinate buildup. We found that 2-DG therapy mitigated CIA pathology by intercepting joint F480 + iNOS + MΦ, Vimentin + fibroblast and CD3 + T cell trafficking along with downregulation of IRFs and glycolytic intermediates. Surprisingly, IACS treatment was inconsequential on CIA swelling, cell infiltration, M1 and Th1/Th17 cytokines (IFN-γ/IL-17) and joint glycolytic mediators. Collectively, our results indicate that blockade of glycolysis is more effective than inhibition of complex 1 in CIA, in part due to its effectiveness on the MΦ inflammatory phenotype., (© 2021. The Author(s), under exclusive licence to Springer Nature Switzerland AG.)

Published

2021

8. Interleukin-34 Reprograms Glycolytic and Osteoclastic Rheumatoid Arthritis Macrophages via Syndecan 1 and Macrophage Colony-Stimulating Factor Receptor.

Author

Van Raemdonck K, Umar S, Palasiewicz K, Volin MV, Elshabrawy HA, Romay B, Tetali C, Ahmed A, Amin MA, Zomorrodi RK, Sweiss N, and Shahrara S

Subjects

Animals, Glycolysis physiology, Inflammation metabolism, Mice, Osteoclasts metabolism, Phosphorylation, Synovial Membrane metabolism, Arthritis, Rheumatoid metabolism, Interleukins metabolism, Macrophages metabolism, Receptor, Macrophage Colony-Stimulating Factor metabolism, Syndecan-1 metabolism

Abstract

Objective: In rheumatoid arthritis (RA), elevated serum interleukin-34 (IL-34) levels are linked with increased disease severity. IL-34 binds to 2 receptors, macrophage colony-stimulating factor receptor (M-CSFR) and syndecan 1, which are coexpressed in RA macrophages. Expression of both IL-34 and syndecan 1 is strikingly elevated in the RA synovium, yet their mechanisms of action remain undefined. This study was undertaken to investigate the mechanism of action of IL-34 in RA., Methods: To characterize the significance of IL-34 in immunometabolism, its mechanism of action was elucidated in joint macrophages, fibroblasts, and T effector cells using RA and preclinical models., Results: Intriguingly, syndecan 1 activated IL-34-induced M-CSFR phosphorylation and reprogrammed RA naive cells into distinctive CD14+CD86+GLUT1+ M34 macrophages that expressed elevated levels of IL-1β, CXCL8, and CCL2. In murine M34 macrophages, the inflammatory phenotype was accompanied by potentiated glycolytic activity, exhibited by transcriptional up-regulation of GLUT1, c-Myc, and hypoxia-inducible factor 1α (HIF-1α) and amplified pyruvate and l-lactate secretion. Local expression of IL-34 provoked arthritis by expanding the glycolytic F4/80-positive, inducible nitric oxide synthase (iNOS)-positive macrophage population, which in turn attracted fibroblasts and polarized Th1/Th17 cells. The cross-talk between murine M34 macrophages and Th1/Th17 cells broadened the inflammatory and metabolic phenotypes, resulting in the expansion of IL-34 pathogenicity. Consequently, IL-34-instigated joint inflammation was alleviated in RAG -/- mice compared to wild-type mice. Syndecan 1 deficiency attenuated IL-34-induced arthritis by interfering with joint glycolytic M34 macrophage and osteoclast remodeling. Similarly, inhibition of glycolysis by 2-deoxy-d-glucose reversed the joint swelling and metabolic rewiring triggered by IL-34 via HIF-1α and c-Myc induction., Conclusion: IL-34 is a novel endogenous factor that remodels hypermetabolic M34 macrophages and facilitates their cross-regulation with T effector cells to advance inflammatory bone destruction in RA., (© 2021, American College of Rheumatology.)

Published

2021

9. IRAK4 inhibition: a promising strategy for treating RA joint inflammation and bone erosion.

Author

Umar S, Palasiewicz K, Van Raemdonck K, Volin MV, Romay B, Amin MA, Zomorrodi RK, Arami S, Gonzalez M, Rao V, Zanotti B, Fox DA, Sweiss N, and Shahrara S

Subjects

Animals, Fibroblasts metabolism, Humans, Inflammation metabolism, Interleukin-1 Receptor-Associated Kinases metabolism, Interleukin-12 metabolism, Tumor Necrosis Factor Inhibitors, Arthritis, Experimental metabolism, Arthritis, Rheumatoid

Abstract

Flares of joint inflammation and resistance to currently available biologic therapeutics in rheumatoid arthritis (RA) patients could reflect activation of innate immune mechanisms. Herein, we show that a TLR7 GU-rich endogenous ligand, miR-Let7b, potentiates synovitis by amplifying RA monocyte and fibroblast (FLS) trafficking. miR-Let7b ligation to TLR7 in macrophages (MΦs) and FLSs expanded the synovial inflammatory response. Moreover, secretion of M1 monokines triggered by miR-Let7b enhanced Th1/Th17 cell differentiation. We showed that IRAK4 inhibitor (i) therapy attenuated RA disease activity by blocking TLR7-induced M1 MΦ or FLS activation, as well as monokine-modulated Th1/Th17 cell polarization. IRAK4i therapy also disrupted RA osteoclastogenesis, which was amplified by miR-Let7b ligation to joint myeloid TLR7. Hence, the effectiveness of IRAK4i was compared with that of a TNF inhibitor (i) or anti-IL-6R treatment in collagen-induced arthritis (CIA) and miR-Let7b-mediated arthritis. We found that TNF or IL-6R blocking therapies mitigated CIA by reducing the infiltration of joint F480 + iNOS + MΦs, the expression of certain monokines, and Th1 cell differentiation. Unexpectedly, these biologic therapies were unable to alleviate miR-Let7b-induced arthritis. The superior efficacy of IRAK4i over anti-TNF or anti-IL-6R therapy in miR-Let7b-induced arthritis or CIA was due to the ability of IRAK4i therapy to restrain the migration of joint F480 + iNOS + MΦs, vimentin + fibroblasts, and CD3 + T cells, in addition to negating the expression of a wide range of monokines, including IL-12, MIP2, and IRF5 and Th1/Th17 lymphokines. In conclusion, IRAK4i therapy may provide a promising strategy for RA therapy by disconnecting critical links between inflammatory joint cells., (© 2020. CSI and USTC.)

Published

2021

10. Tofacitinib therapy intercepts macrophage metabolic reprogramming instigated by SARS-CoV-2 Spike protein.

Author

Palasiewicz K, Umar S, Romay B, Zomorrodi RK, and Shahrara S

Subjects

Arthritis, Rheumatoid metabolism, COVID-19 metabolism, Cells, Cultured, Fibroblasts drug effects, Fibroblasts metabolism, Humans, Interleukin-6 metabolism, Macrophages metabolism, Receptors, Interleukin-6 metabolism, STAT1 Transcription Factor metabolism, STAT3 Transcription Factor metabolism, Signal Transduction drug effects, Tumor Necrosis Factor-alpha metabolism, Macrophages drug effects, Piperidines pharmacology, Pyrimidines pharmacology, SARS-CoV-2 drug effects, Spike Glycoprotein, Coronavirus metabolism, COVID-19 Drug Treatment

Abstract

The molecular mechanism of severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) Spike protein was characterized to identify novel therapies. The impact of tofacitinib, IL-6R Ab, or TNFi therapy was determined on Spike protein or LPS/IFN-γ-induced signaling, inflammation, and metabolic reprogramming in MΦs and/or rheumatoid arthritis (RA) fibroblast-like synoviocyte (FLS). ACE2 frequency was markedly expanded in MΦs compared to T cells and RA FLS. Tofacitinib suppresses Spike protein potentiated STAT1 signaling, whereas this function was unchanged by TNFi. Tofacitinib impairs IL-6/IFN/LPS-induced STAT1 and STAT3 phosphorylation in RA MΦs and FLS. Interestingly, tofacitinib had a broader inhibitory effect on the monokines, glycolytic regulators, or oxidative metabolites compared to IL-6R Ab and TNFi in Spike-protein-activated MΦs. In contrast, all three therapies disrupted IFN-α and IFN-β secretion in response to Spike protein; nonetheless, the IFN-γ was only curtailed by tofacitinib or IL-6R Ab. While tofacitinib counteracted MΦ metabolic rewiring instigated by Spike protein, it was inconsequential on the glycolysis expansion mediated via HK2 and/or LDHA in the activated RA MΦ and FLS. Nevertheless, the potentiated inflammatory response and the diminished oxidative phosphorylation modulated by Spike protein and/or LPS/IFN-γ stimulation in MΦs or RA FLS were reversed by tofacitinib. In conclusion, tofacitinib suppresses MΦ inflammation and immunometabolism triggered by Spike protein and may provide a promising strategy for COVID-19 patients., (© 2021 Wiley-VCH GmbH.)

Published

2021

11. CCL25 and CCR9 is a unique pathway that potentiates pannus formation by remodeling RA macrophages into mature osteoclasts.

Author

Umar S, Palasiewicz K, Van Raemdonck K, Volin MV, Romay B, Ahmad I, Tetali C, Sweiss N, Amin MA, Zomorrodi RK, and Shahrara S

Subjects

Arthritis, Rheumatoid metabolism, Arthritis, Rheumatoid pathology, Cells, Cultured, Chemokine CCL2 immunology, Chemokine CCL2 metabolism, Chemokines, CC metabolism, Extracellular Signal-Regulated MAP Kinases metabolism, Fibroblasts cytology, Fibroblasts immunology, Fibroblasts metabolism, Humans, Interleukin-8 immunology, Interleukin-8 metabolism, Macrophages cytology, Macrophages metabolism, Monocytes cytology, Monocytes immunology, Monocytes metabolism, Osteoclasts cytology, Osteoclasts metabolism, Phosphorylation, Receptors, CCR metabolism, Signal Transduction immunology, Synovial Fluid cytology, Synovial Fluid immunology, Synovial Fluid metabolism, p38 Mitogen-Activated Protein Kinases metabolism, Arthritis, Rheumatoid immunology, Cell Differentiation immunology, Chemokines, CC immunology, Macrophages immunology, Osteoclasts immunology, Receptors, CCR immunology

Abstract

This study elucidates the mechanism of CCL25 and CCR9 in rheumatoid arthritis (RA). RA synovial fluid (SF) expresses elevated levels of CCL25 compared to OA SF and plasma from RA and normal. CCL25 was released into RA SF by fibroblasts (FLS) and macrophages (MΦs) stimulated with IL-1β and IL-6. CCR9 is also presented on IL-1β and IL-6 activated RA FLS and differentiated MΦs. Conversely, in RA PBMCs neither CCL25 nor CCR9 are impacted by 3-month longitudinal TNF inhibitor therapy. CCL25 amplifies RA FLS and monocyte infiltration via p38 and ERK phosphorylation. CCL25-stimulated RA FLS secrete potentiated levels of IL-8 which is disrupted by p38 and ERK inhibitors. CCL25 polarizes RA monocytes into nontraditional M1 MΦs that produce IL-8 and CCL2. Activation of p38 and ERK cascades are also responsible for the CCL25-induced M1 MΦ development. Unexpectedly, CCL25 was unable to polarize RA PBMCs into effector Th1/Th17 cells. Consistently, lymphokine like RANKL was uninvolved in CCL25-induced osteoclastogenesis; however, this manifestation was regulated by osteoclastic factors such as RANK, cathepsin K (CTSK), and TNF-α. In short, we reveal that CCL25/CCR9 manipulates RA FLS and MΦ migration and inflammatory phenotype in addition to osteoclast formation via p38 and ERK activation., (© 2021 Wiley-VCH GmbH.)

Published

2021

12. TLR7 endogenous ligands remodel glycolytic macrophages and trigger skin-to-joint crosstalk in psoriatic arthritis.

Author

Van Raemdonck K, Umar S, Palasiewicz K, Romay B, Volkov S, Arami S, Sweiss N, and Shahrara S

Subjects

Animals, Antigens, CD immunology, Antigens, Differentiation, Myelomonocytic immunology, Cytokines immunology, Humans, Inflammation immunology, Ligands, Lymphocytes immunology, Mice, Mice, Inbred DBA, MicroRNAs immunology, Myeloid Cells immunology, Osteoclasts immunology, Signal Transduction immunology, Synovial Fluid immunology, Th1 Cells immunology, Arthritis, Psoriatic immunology, Joints immunology, Macrophages immunology, Skin immunology, Toll-Like Receptor 7 immunology

Abstract

Thirty percent of psoriasis patients develop psoriatic arthritis (PsA), nevertheless the mechanism remains unknown. Endogenous GU-rich miRNAs activate endosomal TLR7 that plays a critical role in autoimmune diseases. We found that endogenous TLR7 ligands, miR-29 and miR-Let7b, were markedly increased in PsA compared to osteoarthritis (OA) synovial fluid (SF)s. We showed that intradermal (i.d.) miR-Let7b injection promoted skin inflammation, which was characterized by amplified Th1 cells, CD68 + M1 macrophages, and transcriptional upregulation of glycolytic mediators, GLUT1, C-MYC, and HIF1α. Expansion of skin Th1 cells driven by miR-Let7b was also linked to elevated M1-associated IRFs. Interestingly, i.d. miR-Let7b administration exacerbated suboptimal joint inflammation along with metabolic reconfiguration of the PsA-like preclinical model. Moreover, TLR7 agonist, R837, potentiated metabolic reprogramming and expression of IL-1β, IL-6, and IL-12 in murine macrophages, enabling myeloid-to-T-cell crosstalk. Consistently, treatment with glycolytic inhibitors, 2-DG and/or HIF1αi, reversed R837-induced metabolic remodeling and disrupted the TLR7-driven inflammatory phenotype in myeloid and lymphoid cells. Similar to miR-Let7b, R837 also differentiates progenitor cells into mature osteoclasts, primarily through RANKL induction. Taken together, this study indicates that TLR7-instigated metabolic rewiring of macrophages and their cross-regulation of T cells connects skin immunopathology to joint inflammation., (© 2020 Wiley-VCH GmbH.)

Published

2021

13. Macrophages are the primary effector cells in IL-7-induced arthritis.

Author

Kim SJ, Chang HJ, Volin MV, Umar S, Van Raemdonck K, Chevalier A, Palasiewicz K, Christman JW, Volkov S, Arami S, Maz M, Mehta A, Zomorrodi RK, Fox DA, Sweiss N, and Shahrara S

Subjects

Animals, Bone Marrow Cells metabolism, Cell Differentiation, Humans, Interferon-gamma metabolism, Lipopolysaccharides, Macrophages metabolism, Mice, Mice, Inbred C57BL, Middle Aged, Myeloid Cells metabolism, Osteoclasts metabolism, Receptors, Interleukin-7 metabolism, Tumor Necrosis Factor-alpha metabolism, Arthritis, Rheumatoid pathology, Interleukin-7 metabolism, Macrophages pathology

Abstract

Synovial macrophages are crucial in the development of joint inflammation and bone damage; however, the pathways that control macrophage remodeling in inflammatory M1 cells or bone-eroding osteoclasts are not fully understood. We determined that elevated IL-7R/CD127 expression is the hallmark of rheumatoid arthritis (RA) M1 macrophages and that these cells are highly responsive to interleukin-7 (IL-7)-driven osteoclastogenesis. We established that lipopolysaccharide (LPS), interferon-γ (IFNγ), and tumor necrosis factor-α (TNFα), the classic M1 macrophage mediators, enhance IL-7R expression in RA and murine macrophages. The local expression of IL-7 provokes arthritis, predominantly through escalating the number of F480 + iNOS + cells rather than CD3 + T cells. Ectopic LPS injection stabilizes IL-7-induced arthritis by increasing myeloid IL-7R expression, in part via IFNγ induction. Hence, in RAG-/- mice, IL-7-mediated arthritis is suppressed because of the reduction in myeloid IL-7R expression due to the lack of IFNγ. Moreover, the amelioration of IL-7-induced arthritis by anti-TNF therapy is due to a decrease in the number of cells in the unique F480 + iNOS + IL-7R + CCL5 + subset, with no impact on the F480 + Arginase + cell or CD3 + T cell frequency. Consistent with the preclinical findings, the findings of a phase 4 study performed with RA patients following 6 months of anti-TNF therapy revealed that IL-7R expression was reduced without affecting the levels of IL-7. This study shifts the paradigm by discovering that IL-7-induced arthritis is dependent on F480 + iNOS + IL-7R + CCL5 + cell function, which activates TH-1 cells to amplify myeloid IL-7R expression and disease severity.

Published

2020

14. CCL21/CCR7 signaling in macrophages promotes joint inflammation and Th17-mediated osteoclast formation in rheumatoid arthritis.

Author

Van Raemdonck K, Umar S, Palasiewicz K, Volkov S, Volin MV, Arami S, Chang HJ, Zanotti B, Sweiss N, and Shahrara S

Subjects

Animals, Arthritis, Rheumatoid blood, Arthritis, Rheumatoid pathology, Biomarkers metabolism, Cell Differentiation, Cell Polarity, Chemotaxis, Female, Humans, Interleukins metabolism, Male, Mice, Mice, Inbred C57BL, Middle Aged, Monocytes pathology, Myeloid Cells metabolism, Osteogenesis, Receptors, CCR7 blood, Signal Transduction, Synovial Fluid metabolism, Up-Regulation, Arthritis, Rheumatoid immunology, Chemokine CCL21 metabolism, Inflammation pathology, Joints pathology, Macrophages metabolism, Osteoclasts pathology, Receptors, CCR7 metabolism, Th17 Cells immunology

Abstract

In rheumatoid arthritis (RA), synovial tissue abundantly expresses CCL21, a chemokine strongly associated with RA susceptibility. In this study, we aimed to characterize the functional significance of CCL21/CCR7 signaling in different phases of RA pathogenesis. We determined that CCR7 is a hallmark of RA M1 synovial fluid (SF) macrophages, and its expression in RA monocytes and in vitro differentiated macrophages is closely associated with disease activity score (DAS28). In early stages of RA, monocytes infiltrate the synovial tissue. However, blockade of SF CCL21 or CCR7 prevents RA SF-mediated monocyte migration. CCR7 expression in the newly migrated macrophages can be accentuated by LPS and IFNγ and suppressed by IL-4 treatment. We also uncovered that CCL21 stimulation increases the number of M1-polarized macrophages (CD14+CD86+), resulting in elevated transcription of IL-6 and IL-23. These CCL21-induced M1 cytokines differentiate naïve T cells to Th17 cells, without affecting Th1 cell polarization. In the erosive stages of disease, CCL21 potentiates RA osteoclastogenesis through M1-driven Th17 polarization. Disruption of this intricate crosstalk, by blocking IL-6, IL-23, or IL-17 function, impairs the osteoclastogenic capacity of CCL21. Consistent with our in vitro findings, we establish that arthritis mediated by CCL21 expands the joint inflammation to bone erosion by connecting the differentiation of M1 macrophages with Th17 cells. Disease progression is further exacerbated by CCL21-induced neovascularization. We conclude that CCL21 is an attractive novel target for RA therapy, as blockade of its function may abrogate erosive arthritis modulated by M1 macrophages and Th17 cell crosstalk.

Published

2020

15. A Tie2-Notch1 signaling axis regulates regeneration of the endothelial bone marrow niche.

Author

Shao L, Sottoriva K, Palasiewicz K, Zhang J, Hyun J, Soni SS, Paik NY, Gao X, Cuervo H, Malik AB, Rehman J, Lucas D, and Pajcini KV

Subjects

Animals, Bone Marrow drug effects, Bone Marrow metabolism, Endothelial Cells drug effects, Fluorouracil pharmacology, Gamma Rays adverse effects, Gene Expression Profiling, Gene Expression Regulation, Hematopoietic Stem Cells cytology, Hematopoietic Stem Cells metabolism, Humans, Mice, Mice, Knockout, Pancytopenia etiology, Pancytopenia metabolism, Pancytopenia pathology, Cellular Microenvironment drug effects, Endothelial Cells physiology, Receptor, Notch1 metabolism, Receptor, TIE-2 metabolism, Regeneration, Signal Transduction drug effects

Abstract

Loss-of-function studies have determined that Notch signaling is essential for hematopoietic and endothelial development. By deleting a single allele of the Notch1 transcriptional activation domain we generated viable, post-natal mice exhibiting hypomorphic Notch signaling. These heterozygous mice, which lack only one copy of the transcriptional activation domain, appear normal and have no endothelial or hematopoietic phenotype, apart from an inherent, cell-autonomous defect in T-cell lineage development. Following chemotherapy, these hypomorphs exhibited severe pancytopenia, weight loss and morbidity. This phenotype was confirmed in an endothelial-specific, loss-of-function Notch1 model system. Ang1, secreted by hematopoietic progenitors after damage, activated endothelial Tie2 signaling, which in turn enhanced expression of Notch ligands and potentiated Notch1 receptor activation. In our heterozygous, hypomorphic model system, the mutant protein that lacks the Notch1 transcriptional activation domain accumulated in endothelial cells and interfered with optimal activity of the wildtype Notch1 transcriptional complex. Failure of the hypomorphic mutant to efficiently drive transcription of key gene targets such as Hes1 and Myc prolonged apoptosis and limited regeneration of the bone marrow niche. Thus, basal Notch1 signaling is sufficient for niche development, but robust Notch activity is required for regeneration of the bone marrow endothelial niche and hematopoietic recovery., (Copyright© 2019 Ferrata Storti Foundation.)

Published

2019

16. IL-11 facilitates a novel connection between RA joint fibroblasts and endothelial cells.

Author

Elshabrawy HA, Volin MV, Essani AB, Chen Z, McInnes IB, Van Raemdonck K, Palasiewicz K, Arami S, Gonzalez M, Ashour HM, Kim SJ, Zhou G, Fox DA, and Shahrara S

Subjects

Arthritis, Rheumatoid pathology, Endothelial Cells pathology, Female, Fibroblasts pathology, Humans, Interleukin-11 Receptor alpha Subunit metabolism, Interleukin-8 metabolism, Joints pathology, Male, Neovascularization, Pathologic pathology, Transendothelial and Transepithelial Migration, Vascular Endothelial Growth Factor A metabolism, Arthritis, Rheumatoid metabolism, Endothelial Cells metabolism, Fibroblasts metabolism, Interleukin-11 metabolism, Joints metabolism, Neovascularization, Pathologic metabolism

Abstract

IL-11 has been detected in inflamed joints; however, its role in the pathogenesis of arthritis is not yet clear. Studies were conducted to characterize the expression and functional significance of IL-11 and IL-11Rα in rheumatoid arthritis (RA). IL-11 levels were elevated in RA synovial fluid (SF) compared to osteoarthritis (OA) SF and plasma from RA, OA and normal individuals (NLs). Morphologic studies established that IL-11 was detected in lining fibroblasts and macrophages in addition to sublining endothelial cells and macrophages at higher levels in RA compared to NL synovial tissues. Since IL-11Rα was exclusively expressed in RA fibroblasts and endothelial cells, macrophages were not involved in IL-11 effector function. Ligation of IL-11 to IL-11Rα strongly provoked fibroblast infiltration into RA joint, while cell proliferation was unaffected by this process. Secretion of IL-8 and VEGF from IL-11 activated RA fibroblasts was responsible for the indirect effect of IL-11 on endothelial cell transmigration and tube formation. Moreover, IL-11 blockade impaired RA SF capacity to elicit endothelial cell transmigration and tube formation. We conclude that IL-11 binding to endothelial IL-11Rα can directly induce RA angiogenesis. In addition, secretion of proangiogenic factors from migrating fibroblasts potentiated by IL-11 can indirectly contribute to RA neovascularization.

Published

2018

17. MAFB enhances oncogenic Notch signaling in T cell acute lymphoblastic leukemia.

Author

Pajcini KV, Xu L, Shao L, Petrovic J, Palasiewicz K, Ohtani Y, Bailis W, Lee C, Wertheim GB, Mani R, Muthusamy N, Li Y, Meijerink JPP, Blacklow SC, Faryabi RB, Cherry S, and Pear WS

Subjects

Animals, Disease Models, Animal, Female, Humans, MafB Transcription Factor genetics, Mice, Mice, Inbred C57BL, Precursor T-Cell Lymphoblastic Leukemia-Lymphoma genetics, Precursor T-Cell Lymphoblastic Leukemia-Lymphoma metabolism, Proto-Oncogene Protein c-ets-2 genetics, Proto-Oncogene Protein c-ets-2 metabolism, Receptor, Notch1 metabolism, Transcription Factors genetics, Transcription Factors metabolism, Tumor Cells, Cultured, Carcinogenesis, Gene Expression Regulation, Leukemic, MafB Transcription Factor metabolism, Precursor T-Cell Lymphoblastic Leukemia-Lymphoma pathology, Receptor, Notch1 genetics, Signal Transduction

Abstract

Activating mutations in the gene encoding the cell-cell contact signaling protein Notch1 are common in human T cell acute lymphoblastic leukemias (T-ALLs). However, expressing Notch1 mutant alleles in mice fails to efficiently induce the development of leukemia. We performed a gain-of-function screen to identify proteins that enhanced signaling by leukemia-associated Notch1 mutants. The transcription factors MAFB and ETS2 emerged as candidates that individually enhanced Notch1 signaling, and when coexpressed, they synergistically increased signaling to an extent similar to that induced by core components of the Notch transcriptional complex. In mouse models of T-ALL, MAFB enhanced leukemogenesis by the naturally occurring Notch1 mutants, decreased disease latency, and increased disease penetrance. Decreasing MAFB abundance in mouse and human T-ALL cells reduced the expression of Notch1 target genes, including MYC and HES1 , and sustained MAFB knockdown impaired T-ALL growth in a competitive setting. MAFB bound to ETS2 and interacted with the acetyltransferases PCAF and P300, highlighting its importance in recruiting coactivators that enhance Notch1 signaling. Together, these data identify a mechanism for enhancing the oncogenic potential of weak Notch1 mutants in leukemia models, and they reveal the MAFB-ETS2 transcriptional axis as a potential therapeutic target in T-ALL., (Copyright © 2017 The Authors, some rights reserved; exclusive licensee American Association for the Advancement of Science. No claim to original U.S. Government Works.)

Published

2017

18. Aging-associated dysregulation of homeostatic immune response termination (and not initiation).

Author

Pattabiraman G, Palasiewicz K, Galvin JP, and Ucker DS

Subjects

Age Factors, Animals, Apoptosis immunology, Gene Expression Regulation, Developmental, Homeostasis genetics, Homeostasis immunology, Humans, Interleukin-10 genetics, Lipopolysaccharides pharmacology, Macrophage Activation drug effects, Macrophages cytology, Macrophages immunology, Mice, Mice, Inbred C57BL, Primary Cell Culture, Signal Transduction, Single-Cell Analysis, Tumor Necrosis Factor-alpha genetics, Immunity, Innate, Immunosenescence genetics, Interleukin-10 immunology, Macrophages drug effects, Transcription, Genetic immunology, Tumor Necrosis Factor-alpha immunology

Abstract

Immunosenescence is a state of unbalanced immune responsiveness, characterized by a diverse repertoire of seemingly discreet and paradoxical alterations in all aspects of immunity arising in an aging-associated manner. We asked whether aging-associated alterations in the ability of apoptotic cells to elicit immunomodulatory responses (innate apoptotic immunity; IAI) or in IAI responses themselves might underlie the confounding aging-associated anomalies of immunosenescence. We explored this question by examining, as a function of animal age, responsiveness of murine macrophages on the single cell level. We monitored the expression of pro- and anti-inflammatory cytokines cytofluorimetrically in response to pro-inflammatory Toll-like receptor (TLR) stimulation and anti-inflammatory treatment with apoptotic cells. While we found no alterations with age in the potency of apoptotic cells or in the initiation and magnitude of IAI responses, we did identify a cell-intrinsic deficiency in anti-inflammatory IAI response termination linked with age and preceding manifestations of immunosenescence. Further, we found that an aging-associated deficiency in response termination also is evident following TLR stimulation. These surprising observations reveal that a loss of homeostatic immune control with animal age results from the dysregulation of response termination (as distinct from response initiation) and is exerted on the level of transcription. We suggest that, with advancing age, cells become locked into relatively longer-lived response states. Aging-associated immune dysfunctions may reflect a diminution in the cellular nimbleness of immune responsiveness., (© 2017 The Authors. Aging Cell published by the Anatomical Society and John Wiley & Sons Ltd.)

Published

2017

19. Apoptotic cells enhance pathogenesis of Listeria monocytogenes.

Author

Pattabiraman G, Palasiewicz K, Visvabharathy L, Freitag NE, and Ucker DS

Subjects

Animals, Cell Line, Cells, Cultured, Cytokines immunology, Disease Models, Animal, Immunity, Innate, Inflammation immunology, Inflammation pathology, Listeria monocytogenes immunology, Listeriosis microbiology, Lymphocytes immunology, Mice, Inbred C57BL, Signal Transduction, Apoptosis immunology, Listeria monocytogenes pathogenicity, Listeriosis immunology, Listeriosis pathology

Abstract

Infections by pathogenic microorganisms elicit host immune responses, which crucially limit those infections. Pathogens employ various strategies to evade host immunity. We have identified the exploitation of the repertoire of potent immunosuppressive responses elicited normally by apoptotic cells ("Innate Apoptotic Immunity"; IAI) as one of these strategies. In the case of Listeria monocytogenes, an environmentally ubiquitous, foodborne bacterial pathogen capable of causing life-threatening invasive disease in immunocompromised and elderly individuals, the induction of host cell apoptosis appears to play an important role in pathogenesis. Previous studies have documented extensive lymphocyte apoptosis resulting from L. monocytogenes infection and demonstrated paradoxically that lymphocyte-deficient animals exhibit diminished susceptibility to listerial pathogenicity. We speculated that the triggering of IAI following the induction of host cell apoptosis was responsible for enhanced pathogenesis, and that the administration of exogenous apoptotic cells would serve to exert this effect. Importantly, apoptotic cells, which are not susceptible to L. monocytogenes infection, do not provide a niche for bacterial replication. Our experiments confirm that apoptotic cells, including exogenous apoptotic cells induced to die independently of the pathogen, specifically enhance pathogenesis. The recognition of a role of apoptotic cells and Innate Apoptotic Immunity in microbial pathogenesis provides an intriguing and novel insight for therapeutic approaches for the control of pathogenic infections., (Copyright © 2017 Elsevier Ltd. All rights reserved.)

Published

2017

20. Toll-like Receptor function of murine macrophages, probed by cytokine induction, is biphasic and is not impaired globally with age.

Author

Pattabiraman G, Palasiewicz K, and Ucker DS

Subjects

Animals, Mice, Mice, Inbred BALB C, Toll-Like Receptors agonists, Aging immunology, Cytokines immunology, Immunity, Innate physiology, Macrophages immunology, Toll-Like Receptors immunology

Abstract

Aging is associated with a waning of normal immune function. This "immunosenescence" is characterized by a diverse repertoire of seemingly discreet and unbalanced immune alterations. A number of studies have suggested that aging-associated alterations in innate immune responsiveness, especially responsiveness dependent on Toll-like Receptor (TLR) engagement, are causally involved. We find, however, that the magnitude and dose-dependency of responsiveness to TLR engagement (assessed with respect to cytokine production) in distinct populations of murine macrophages are not altered generally with animal age or as a consequence of immunosenescence. Responses elicited with a wide array of TLR agonists were examined by extensive functional analyses, principally on the level of the individual cell. These studies reveal an intriguing "all-or-nothing" response behavior of macrophages, independent of animal age. Although reports to the contrary have been cited widely, aging-associated immune decline cannot be attributed to widespread alterations in the extents of TLR-dependent innate immune macrophage responses., Competing Interests: The authors declare that they have no conflicts or competing commercial interests in relation to this work., (Copyright © 2016 Elsevier Ireland Ltd. All rights reserved.)

Published

2016

21. Recognition of apoptotic cells by viable cells is specific, ubiquitous, and species independent: analysis using photonic crystal biosensors.

Author

Pattabiraman G, Lidstone EA, Palasiewicz K, Cunningham BT, and Ucker DS

Subjects

Animals, Cell Adhesion, Cell Communication, Cell Survival, Crystallization, Cytoskeleton metabolism, Humans, Jurkat Cells, Mice, Phagocytosis, Species Specificity, Apoptosis, Biosensing Techniques methods, Photons

Abstract

Apoptotic recognition is innate and linked to a profound immune regulation (innate apoptotic immunity [IAI]) involving anti-inflammatory and immunosuppressive responses. Many of the molecular and mechanistic details of this response remain elusive. Although immune outcomes can be quantified readily, the initial specific recognition events have been difficult to assess. We developed a sensitive, real-time method to detect the recognition of apoptotic cells by viable adherent responder cells, using a photonic crystal biosensor approach. The method relies on characteristic spectral shifts resulting from the specific recognition and dose-dependent interaction of adherent responder cells with nonadherent apoptotic targets. Of note, the biosensor provides a readout of early recognition-specific events in responder cells that occur distal to the biosensor surface. We find that innate apoptotic cell recognition occurs in a strikingly species-independent manner, consistent with our previous work and inferences drawn from indirect assays. Our studies indicate obligate cytoskeletal involvement, although apoptotic cell phagocytosis is not involved. Because it is a direct, objective, and quantitative readout of recognition exclusively, this biosensor approach affords a methodology with which to dissect the early recognition events associated with IAI and immunosuppression., (© 2014 Pattabiraman et al. This article is distributed by The American Society for Cell Biology under license from the author(s). Two months after publication it is available to the public under an Attribution–Noncommercial–Share Alike 3.0 Unported Creative Commons License (http://creativecommons.org/licenses/by-nc-sa/3.0).)

Published

2014

22. Externalized glycolytic enzymes are novel, conserved, and early biomarkers of apoptosis.

Author

Ucker DS, Jain MR, Pattabiraman G, Palasiewicz K, Birge RB, and Li H

Subjects

Animals, Biomarkers metabolism, Humans, Jurkat Cells, Lupus Erythematosus, Systemic enzymology, Lupus Erythematosus, Systemic pathology, Mice, Proteomics, U937 Cells, Apoptosis, Glycolysis, Immunity, Innate

Abstract

The intriguing cell biology of apoptotic cell death results in the externalization of numerous autoantigens on the apoptotic cell surface, including protein determinants for specific recognition, linked to immune responses. Apoptotic cells are recognized by phagocytes and trigger an active immunosuppressive response ("innate apoptotic immunity" (IAI)) even in the absence of engulfment. IAI is responsible for the lack of inflammation associated normally with the clearance of apoptotic cells; its failure also has been linked to inflammatory and autoimmune pathology, including systemic lupus erythematosus and rheumatic diseases. Apoptotic recognition determinants underlying IAI have yet to be identified definitively; we argue that these molecules are surface-exposed (during apoptotic cell death), ubiquitously expressed, protease-sensitive, evolutionarily conserved, and resident normally in viable cells (SUPER). Using independent and unbiased quantitative proteomic approaches to characterize apoptotic cell surface proteins and identify candidate SUPER determinants, we made the surprising discovery that components of the glycolytic pathway are enriched on the apoptotic cell surface. Our data demonstrate that glycolytic enzyme externalization is a common and early aspect of cell death in different cell types triggered to die with distinct suicidal stimuli. Exposed glycolytic enzyme molecules meet the criteria for IAI-associated SUPER determinants. In addition, our characterization of the apoptosis-specific externalization of glycolytic enzyme molecules may provide insight into the significance of previously reported cases of plasminogen binding to α-enolase on mammalian cells, as well as mechanisms by which commensal bacteria and pathogens maintain immune privilege.

Published

2012